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Proteasomal selection of multiprotein complexes recruited by LIM homeodomain transcription factors

机译:LIM同源域转录因子募集的多蛋白复合物的蛋白酶体选择

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摘要

Complexes composed of multiple proteins regulate most cellular functions. However, our knowledge about the molecular mechanisms governing the assembly and dynamics of these complexes in cells remains limited. The in vivo activity of LIM homeodomain (LIM-HD) proteins, a class of transcription factors that regulates neuronal development, depends on the high-affinity association of their LIM domains with cofactor of LIM homeodomain proteins (LIM-HDs) (CLIM, also known as Ldb or NLI). CLIM cofactors recruit single-stranded DNA-binding protein 1 (SSDP1, also known as SδBP3), and this interaction is important for the activation of the LIM-HD/CLIM protein complex in vivo. Here, we identify a cascade of specific protein interactions that protect LIM-HD multiprotein complexes from proteasomal degradation. In this cascade, CLIM stabilizes LIM-HDs, and SSDP1 stabilizes CLIM. Furthermore, we show that stabilizing cofactors prevent binding of ubiquitin ligases to multiple protein interaction domains in LIM-HD recruited protein complexes. Together, our results indicate a combinatorial code that selects specific multiprotein complexes via proteasomal degradation in cells with broad implications for the assembly and specificity of multiprotein complexes.
机译:由多种蛋白质组成的复合物调节大多数细胞功能。但是,我们对控制这些复合物在细胞中的组装和动力学的分子机制的知识仍然有限。 LIM同源域(LIM-HD)蛋白是一类调节神经元发育的转录因子,其体内活性取决于其LIM域与LIM同源域蛋白(LIM-HDs)(CLIM,称为Ldb或NLI)。 CLIM辅助因子募集单链DNA结合蛋白1(SSDP1,也称为SδBP3),这种相互作用对于体内LIM-HD / CLIM蛋白复合物的激活很重要。在这里,我们确定了一系列特定的蛋白质相互作用,可以保护LIM-HD多蛋白复合物免受蛋白酶体降解。在此级联中,CLIM稳定LIM-HD,SSDP1稳定CLIM。此外,我们显示稳定的辅助因子可防止泛素连接酶与LIM-HD募集的蛋白质复合物中的多个蛋白质相互作用域结合。在一起,我们的结果表明组合代码,通过细胞中的蛋白酶体降解来选择特定的多蛋白复合物,对多蛋白复合物的组装和特异性具有广泛的意义。

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